APOBEC3A and APOBEC3B Preferentially Deaminate the Lagging Strand Template during DNA Replication

doi:10.1016/j.celrep.2016.01.021

. 2016 Feb 16;14(6):1273-1282.

doi: 10.1016/j.celrep.2016.01.021. Epub 2016 Jan 28.

APOBEC3A and APOBEC3B Preferentially Deaminate the Lagging Strand Template during DNA Replication

James I Hoopes¹, Luis M Cortez¹, Tony M Mertz¹, Ewa P Malc², Piotr A Mieczkowski², Steven A Roberts³

Affiliations

¹ School of Molecular Biosciences, College of Veterinary Medicine, Washington State University, Pullman, WA 99164, USA.
² Department of Genetics, Lineberger Comprehensive Cancer Center, University of North Carolina, Chapel Hill, NC 27599, USA.
³ School of Molecular Biosciences, College of Veterinary Medicine, Washington State University, Pullman, WA 99164, USA. Electronic address: sroberts@vetmed.wsu.edu.

PMID: 26832400
PMCID: PMC4758883
DOI: 10.1016/j.celrep.2016.01.021

APOBEC3A and APOBEC3B Preferentially Deaminate the Lagging Strand Template during DNA Replication

James I Hoopes et al. Cell Rep. 2016.

. 2016 Feb 16;14(6):1273-1282.

doi: 10.1016/j.celrep.2016.01.021. Epub 2016 Jan 28.

Authors

James I Hoopes¹, Luis M Cortez¹, Tony M Mertz¹, Ewa P Malc², Piotr A Mieczkowski², Steven A Roberts³

Affiliations

¹ School of Molecular Biosciences, College of Veterinary Medicine, Washington State University, Pullman, WA 99164, USA.
² Department of Genetics, Lineberger Comprehensive Cancer Center, University of North Carolina, Chapel Hill, NC 27599, USA.
³ School of Molecular Biosciences, College of Veterinary Medicine, Washington State University, Pullman, WA 99164, USA. Electronic address: sroberts@vetmed.wsu.edu.

PMID: 26832400
PMCID: PMC4758883
DOI: 10.1016/j.celrep.2016.01.021

Abstract

APOBEC family cytidine deaminases have recently been implicated as powerful mutators of cancer genomes. How APOBECs, which are ssDNA-specific enzymes, gain access to chromosomal DNA is unclear. To ascertain the chromosomal ssDNA substrates of the APOBECs, we expressed APOBEC3A and APOBEC3B, the two most probable APOBECs mediating cancer mutagenesis, in a yeast model system. We demonstrate, using mutation reporters and whole genome sequencing, that APOBEC3A- and APOBEC3B-induced mutagenesis primarily results from the deamination of the lagging strand template during DNA replication. Moreover, our results indicate that both genetic deficiencies in replication fork-stabilizing proteins and chemical induction of replication stress greatly augment the mutagenesis of APOBEC3A and APOBEC3B. Taken together, these results strongly indicate that ssDNA formed during DNA lagging strand synthesis is a major substrate for APOBECs and may be the principal substrate in human cancers experiencing replication stress.

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Figures

**Figure 1. APOBEC3A and 3B induce strand-bias mutations around ARS216**
(A) Frequencies of canavanine-resistance (Can^R) induced in WT and *ung1*Δ yeast following transformation with vector control plasmid, A3A expression plasmid, or A3B expression plasmid. Can^R frequency was determined in isogenic strains with the *CAN1* gene located either 16 kB 5′ of the origin of replication, ARS216, or 7 kB 3′ of ARS216. Horizontal bars and numeric values indicate the median frequency of six or seven independent replicates. Statistical significance was determined by two-tailed non-parametric Mann-Whitney Rank test. See also **Figure S1**. (B) Sequence logo describing the favored trinucleotide sequences mutated by A3A (top) and A3B (bottom) in *ung1*Δ yeast. See also **Table S1**. (C) Specific deamination of ssDNA formed in a transcription bubble would result in C to T transitions (red ball) within *CAN1* regardless of whether the gene is positioned 5′ or 3′ of ARS216. In contrast, deamination of ssDNA formed during lagging strand synthesis would result in G to A substitutions (green ball) 5′ and C to T substitutions 3′ or the origin. (D) The number of G to A (green) and C to T (red) substitutions induced in the *CAN1* gene (located 5′ and 3′ of ARS216) by A3A and A3B in *ung1*Δ and *UNG1* yeast as determined by sequencing independent Can^R isolates. P-values were determined using a one-tailed g-test goodness-of-fit comparing the ratio of C to T substitutions to G to A substitutions to an expected 1:1 ratio. See also **Table S1**.

**Figure 2. Genome-wide strand-bias of A3A and A3B mutations between neighboring origins of replication**
(A) Distribution of C to T (red) and G to A (green) mutations induced by A3A (top) and A3B (bottom). Yeast chromosomes are displayed in gray. (B) The relative abundance of A3A- and A3B-induced C to T mutations (red) and G to A mutations (green) in yeast genes +/− 500 nucleotides transcribed on the bottom strand (B) or the top strand (T). P-values were determined using a two-tailed chi-square test comparing the numbers of each mutation type to the number of A3A- and A3B-targeted TC (red) or GA (green) dinucleotides occurring in these regions. (C) The relative abundance of A3A- and A3B-induced C to T mutations (red) and G to A mutations (green) according to the fractional distance between neighboring replication origins. Lines represent linear trend lines fitting the fractional abundance of C to T (red) and G to A (green) mutations across the entire fractional distance between neighboring origins. A statistical significance of p<0.0001 was determined by comparing the number of each mutation type in each decile bin to the corresponding abundance of TC or GA dinucleotides, by chi-square test. See also **Table S2**.

**Figure 3. Deletion of replication fork stability factors exacerbates A3A- and A3B-induced mutagenesis around ARS216**
(A) Frequencies of Can^R induced in wild type, *rfa1-t33, tof1*Δ, *ung1*Δ, *rfa1-t33 ung1*Δ, and *tof1*Δ *ung1*Δ yeast following transformation with vector control plasmid, A3A expression plasmid, or A3B expression plasmid. Horizontal bars and numeric values indicate the median frequency of six or seven independent replicates. P-values were determined by two-tailed non-parametric Mann-Whitney Rank test. (B) The number of G to A (green) and C to T (red) substitutions induced in the *CAN1* gene (located 5′ and 3′ of ARS216) by A3A and A3B in *ung1*Δ yeast in the genetic backgrounds mentioned in (A) as determined by sequencing independent Can^R isolates. P-values were determined using a two-tailed Fisher's Exact test comparing the ratio of C to T substitutions to G to A substitutions between indicated genotypes. See also **Table S1**.

**Figure 4. Chemically-induced replication stress augments A3A- and A3B-induced mutagenesis**
(A) HU treatment causes a dose-dependent decrease in cell growth in *ung1*Δ yeast. Shown are medians and ranges for 18 independent replicates at each HU dose. P-values were determined by two-tailed non-parametric Mann-Whitney Rank test comparing untreated yeast to yeast treated with 50 mM HU. (B) Frequencies of Can^R induced in *ung1*Δ yeast treated with 0, 12.5, 25, or 50 mM HU following transformation with vector control plasmid, A3A expression plasmid, or A3B expression plasmid. Horizontal bars and numeric values indicate the median frequency of six or seven independent replicates. P-values were determined by two-tailed non-parametric Mann-Whitney Rank test. (C) The number of G to A (green) and C to T (red) substitutions induced in the *CAN1* gene by A3A and A3B in untreated or 50mM HU treated *ung1*Δ yeast as determined by sequencing independent Can^R isolates. P-values were determined using a two-tailed Fisher's Exact test comparing the ratio of C to T substitutions to G to A substitutions between indicated treatments. See also **Table S1**.

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References

1. ALEXANDROV LB, NIK-ZAINAL S, WEDGE DC, APARICIO SA, BEHJATI S, BIANKIN AV, BIGNELL GR, BOLLI N, BORG A, BORRESEN-DALE AL, BOYAULT S, BURKHARDT B, BUTLER AP, CALDAS C, DAVIES HR, DESMEDT C, EILS R, EYFJORD JE, FOEKENS JA, GREAVES M, HOSODA F, HUTTER B, ILICIC T, IMBEAUD S, IMIELINSK M, JAGER N, JONES DT, JONES D, KNAPPSKOG S, KOOL M, LAKHANI SR, LOPEZ-OTIN C, MARTIN S, MUNSHI NC, NAKAMURA H, NORTHCOTT PA, PAJIC M, PAPAEMMANUIL E, PARADISO A, PEARSON JV, PUENTE XS, RAINE K, RAMAKRISHNA M, RICHARDSON AL, RICHTER J, ROSENSTIEL P, SCHLESNER M, SCHUMACHER TN, SPAN PN, TEAGUE JW, TOTOKI Y, TUTT AN, VALDES-MAS R, VAN BUUREN MM, VAN 'T VEER L, VINCENT-SALOMON A, WADDELL N, YATES LR, ZUCMAN-ROSSI J, FUTREAL PA, MCDERMOTT U, LICHTER P, MEYERSON M, GRIMMOND SM, SIEBERT R, CAMPO E, SHIBATA T, PFISTER SM, CAMPBELL PJ, STRATTON MR. Signatures of mutational processes in human cancer. Nature. 2013;500:415–21. - PMC - PubMed
1. BALAKRISHNAN L, BAMBARA RA. Eukaryotic lagging strand DNA replication employs a multi-pathway mechanism that protects genome integrity. J Biol Chem. 2011;286:6865–70. - PMC - PubMed
1. BELLI G, GARI E, PIEDRAFITA L, ALDEA M, HERRERO E. An activator/repressor dual system allows tight tetracycline-regulated gene expression in budding yeast. Nucleic Acids Res. 1998;26:942–7. - PMC - PubMed
1. BHAGWAT AS, HAO W, TOWNES JP, LEE H, TANG H, FOSTER PL. Strand-biased Cytosine deamination at the Replication Fork causes Cytosine to Thymine Mutations in Escherichia coli. PNAS. 2016 - PMC - PubMed
1. BIANCHI V, PONTIS E, REICHARD P. Changes of deoxyribonucleoside triphosphate pools induced by hydroxyurea and their relation to DNA synthesis. J Biol Chem. 1986;261:16037–42. - PubMed

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[1] ALEXANDROV LB, NIK-ZAINAL S, WEDGE DC, APARICIO SA, BEHJATI S, BIANKIN AV, BIGNELL GR, BOLLI N, BORG A, BORRESEN-DALE AL, BOYAULT S, BURKHARDT B, BUTLER AP, CALDAS C, DAVIES HR, DESMEDT C, EILS R, EYFJORD JE, FOEKENS JA, GREAVES M, HOSODA F, HUTTER B, ILICIC T, IMBEAUD S, IMIELINSK M, JAGER N, JONES DT, JONES D, KNAPPSKOG S, KOOL M, LAKHANI SR, LOPEZ-OTIN C, MARTIN S, MUNSHI NC, NAKAMURA H, NORTHCOTT PA, PAJIC M, PAPAEMMANUIL E, PARADISO A, PEARSON JV, PUENTE XS, RAINE K, RAMAKRISHNA M, RICHARDSON AL, RICHTER J, ROSENSTIEL P, SCHLESNER M, SCHUMACHER TN, SPAN PN, TEAGUE JW, TOTOKI Y, TUTT AN, VALDES-MAS R, VAN BUUREN MM, VAN 'T VEER L, VINCENT-SALOMON A, WADDELL N, YATES LR, ZUCMAN-ROSSI J, FUTREAL PA, MCDERMOTT U, LICHTER P, MEYERSON M, GRIMMOND SM, SIEBERT R, CAMPO E, SHIBATA T, PFISTER SM, CAMPBELL PJ, STRATTON MR. Signatures of mutational processes in human cancer. Nature. 2013;500:415–21. - PMC - PubMed

[2] ALEXANDROV LB, NIK-ZAINAL S, WEDGE DC, APARICIO SA, BEHJATI S, BIANKIN AV, BIGNELL GR, BOLLI N, BORG A, BORRESEN-DALE AL, BOYAULT S, BURKHARDT B, BUTLER AP, CALDAS C, DAVIES HR, DESMEDT C, EILS R, EYFJORD JE, FOEKENS JA, GREAVES M, HOSODA F, HUTTER B, ILICIC T, IMBEAUD S, IMIELINSK M, JAGER N, JONES DT, JONES D, KNAPPSKOG S, KOOL M, LAKHANI SR, LOPEZ-OTIN C, MARTIN S, MUNSHI NC, NAKAMURA H, NORTHCOTT PA, PAJIC M, PAPAEMMANUIL E, PARADISO A, PEARSON JV, PUENTE XS, RAINE K, RAMAKRISHNA M, RICHARDSON AL, RICHTER J, ROSENSTIEL P, SCHLESNER M, SCHUMACHER TN, SPAN PN, TEAGUE JW, TOTOKI Y, TUTT AN, VALDES-MAS R, VAN BUUREN MM, VAN 'T VEER L, VINCENT-SALOMON A, WADDELL N, YATES LR, ZUCMAN-ROSSI J, FUTREAL PA, MCDERMOTT U, LICHTER P, MEYERSON M, GRIMMOND SM, SIEBERT R, CAMPO E, SHIBATA T, PFISTER SM, CAMPBELL PJ, STRATTON MR. Signatures of mutational processes in human cancer. Nature. 2013;500:415–21. - PMC - PubMed

[3] BALAKRISHNAN L, BAMBARA RA. Eukaryotic lagging strand DNA replication employs a multi-pathway mechanism that protects genome integrity. J Biol Chem. 2011;286:6865–70. - PMC - PubMed

[4] BALAKRISHNAN L, BAMBARA RA. Eukaryotic lagging strand DNA replication employs a multi-pathway mechanism that protects genome integrity. J Biol Chem. 2011;286:6865–70. - PMC - PubMed

[5] BELLI G, GARI E, PIEDRAFITA L, ALDEA M, HERRERO E. An activator/repressor dual system allows tight tetracycline-regulated gene expression in budding yeast. Nucleic Acids Res. 1998;26:942–7. - PMC - PubMed

[6] BELLI G, GARI E, PIEDRAFITA L, ALDEA M, HERRERO E. An activator/repressor dual system allows tight tetracycline-regulated gene expression in budding yeast. Nucleic Acids Res. 1998;26:942–7. - PMC - PubMed

[7] BHAGWAT AS, HAO W, TOWNES JP, LEE H, TANG H, FOSTER PL. Strand-biased Cytosine deamination at the Replication Fork causes Cytosine to Thymine Mutations in Escherichia coli. PNAS. 2016 - PMC - PubMed

[8] BHAGWAT AS, HAO W, TOWNES JP, LEE H, TANG H, FOSTER PL. Strand-biased Cytosine deamination at the Replication Fork causes Cytosine to Thymine Mutations in Escherichia coli. PNAS. 2016 - PMC - PubMed

[9] BIANCHI V, PONTIS E, REICHARD P. Changes of deoxyribonucleoside triphosphate pools induced by hydroxyurea and their relation to DNA synthesis. J Biol Chem. 1986;261:16037–42. - PubMed

[10] BIANCHI V, PONTIS E, REICHARD P. Changes of deoxyribonucleoside triphosphate pools induced by hydroxyurea and their relation to DNA synthesis. J Biol Chem. 1986;261:16037–42. - PubMed

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APOBEC3A and APOBEC3B Preferentially Deaminate the Lagging Strand Template during DNA Replication

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APOBEC3A and APOBEC3B Preferentially Deaminate the Lagging Strand Template during DNA Replication

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